Author:
Kringelbach Tina,Højgaard Martin,Rohrberg Kristoffer,Spanggaard Iben,Laursen Britt Elmedal,Ladekarl Morten,Haslund Charlotte Aaquist,Harsløf Laurine,Belcaid Laila,Gehl Julie,Søndergaard Lise,Eefsen Rikke Løvendahl,Hansen Karin Holmskov,Kodahl Annette Raskov,Jensen Lars Henrik,Holt Marianne Ingerslev,Oellegaard Trine Heide,Yde Christina Westmose,Ahlborn Lise Barlebo,Lassen Ulrik
Abstract
AbstractBackgroundAn increasing number of trials indicate that treatment outcomes in cancer patients with metastatic disease are improved when targeted treatments are matched with druggable genomic alterations in individual patients (pts). An estimated 30–80% of advanced solid tumors harbor actionable genomic alterations. However, the efficacy of personalized cancer treatment is still scarcely investigated in larger, controlled trials due to the low frequency and heterogenous distribution of druggable alterations among different histologic tumor types. Therefore, the overall effect of targeted cancer treatment on clinical outcomes still needs investigation.Study design/methodsProTarget is a national, non-randomized, multi-drug, open-label, pan-cancer phase 2 trial aiming to investigate the anti-tumor activity and toxicity of currently 13 commercially available, EMA-approved targeted therapies outside the labeled indication for treatment of advanced malignant diseases, harboring specific actionable genomic alterations. The trial involves the Danish National Molecular Tumor Board for confirmation of drug-variant matches. Key inclusion criteria include a) measurable disease (RECIST v.1.1), b) ECOG performance status 0–2, and c) an actionable genomic alteration matching one of the study drugs. Key exclusion criteria include a) cancer type within the EMA-approved label of the selected drug, and b) genomic alterations known to confer drug resistance. Initial drug dose, schedule and dose modifications are according to the EMA-approved label. The primary endpoint is objective response or stable disease at 16 weeks. Pts are assigned to cohorts defined by the selected drug, genomic alteration, and tumor histology type. Cohorts are monitored according to a Simon’s two-stage-based design. Response is assessed every 8 weeks for the first 24 weeks, then every 12 weeks. The trial is designed similar to the Dutch DRUP and the ASCO TAPUR trials and is a partner in the Nordic Precision Cancer Medicine Trial Network. In ProTarget, serial fresh tumor and liquid biopsies are mandatory and collected for extensive translational research including whole genome sequencing, array analysis, and RNA sequencing.DiscussionThe ProTarget trial will identify new predictive biomarkers for targeted treatments and provide new data and essential insights in molecular pathways involved in e.g., resistance mechanisms and thereby potentially evolve and expand the personalized cancer treatment strategy.Protocol version: 16, 09-MAY-2022.Trial registrationClinicalTrials.gov Identifier: NCT04341181.Secondary Identifying No: ML41742.EudraCT No: 2019–004771-40.
Publisher
Springer Science and Business Media LLC
Subject
Cancer Research,Genetics,Oncology